| Literature DB >> 26997761 |
Michal A Rahat1, Jivan Shakya1.
Abstract
Cancer and autoimmune diseases are fundamentally different pathological conditions. In cancer, the immune response is suppressed and unable to eradicate the transformed self-cells, while in autoimmune diseases it is hyperactivated against a self-antigen, leading to tissue injury. Yet, mechanistically, similarities in the triggering of the immune responses can be observed. In this review, we highlight some parallel aspects of the microenvironment in cancer and autoimmune diseases, especially hypoxia, and the role of macrophages, neutrophils, and their interaction. Macrophages, owing to their plastic mode of activation, can generate a pro- or antitumoral microenvironment. Similarly, in autoimmune diseases, macrophages tip the Th1/Th2 balance via various effector cytokines. The contribution of neutrophils, an additional plastic innate immune cell population, to the microenvironment and disease progression is recently gaining more prominence in both cancer and autoimmune diseases, as they can secrete cytokines, chemokines, and reactive oxygen species (ROS), as well as acquire an enhanced ability to produce neutrophil extracellular traps (NETs) that are now considered important initiators of autoimmune diseases. Understanding the contribution of macrophages and neutrophils to the cancerous or autoimmune microenvironment, as well as the role their interaction and cooperation play, may help identify new targets and improve therapeutic strategies.Entities:
Mesh:
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Year: 2016 PMID: 26997761 PMCID: PMC4779817 DOI: 10.1155/2016/4375120
Source DB: PubMed Journal: Mediators Inflamm ISSN: 0962-9351 Impact factor: 4.711
Hypoxia in the microenvironment.
| Cancer tissue | RA (SF) | MS/EAE | SLE | |
|---|---|---|---|---|
| Hypoxia | ≤5 mmHg (70–80 | 18–24 mmHg | 9–20 mmHg in EAE [ | Not directly measured; |
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| Normal tissue | Range: 25–72 mmHg (depending on tissue) [ | 40–70 mmHg [ | 35 mmHg [ | |
Examples for the distribution of macrophages and neutrophils in different types of cancer and autoimmune diseases.
| Type of carcinoma | Localization | Percentage (%) | Mice/human | Ref |
|---|---|---|---|---|
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| Mammary gland | Macrophages are found infiltrating all areas of the tumors (including the perinecroptic areas) | >40% | Mice | [ |
| Prostate cancer | In stroma and in close contact with cancer cells | 10%–15% | Human | [ |
| Pancreatic cancer | Intratumoral and in the invasive front | 30–50% | Human | [ |
| Colon cancer | Intratumoral, numbers increase with tumor stage and grade | 25%–50% | Human | [ |
| L929 Fibrosarcoma, B16 melanoma, LLC lung carcinoma cells | Intratumoral | 23–51% | Mice | [ |
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| Lung cancer | Infiltrating the tumor | 8% | Human | [ |
| Clear cell renal cell carcinoma (RCC) | Intratumoral or near vessels | 14% | Human | [ |
| Mesothelioma, lung cancer | Intratumoral | 0.7–2.5% | Mice | [ |
| L929 Fibrosarcoma, B16 melanoma, LLC lung carcinoma cells | Intratumoral or near vessels | 3–8% | Mice | [ |
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| Rheumatoid arthritis (RA) | Lining the synovial membrane | 41% | Human | [ |
| Lining and infiltrating the synovium | 35–46% | Human | [ | |
| Lining and infiltrating the synovium | 17–36% | Human | [ | |
| Infiltrating the synovium | 26% | Human | [ | |
| Multiple sclerosis (MS) | Infiltrating and at the rim of the lesion | 15–30% | Human | [ |
| Systemic lupus (SLE) | Kidney: infiltrating all parenchyma, found surrounding glomeruli and around perivascular aggregate | 26% | Mice | [ |
| Systemic lupus (SLE) | Throughout the nephritic kidney | 4% | Mice | [ |
| Scleroderma | Skin | 23% | Rat | [ |
| Systemic sclerosis (SSc) | Superficial and deep dermis at early stages | 13% | Human | [ |
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| Rheumatoid arthritis (RA) | Lining and infiltrating the synovium | 8–15% | Human | [ |
| Infiltrating the synovium | 4.5–7% | Human | [ | |
| Experimental autoimmune encephalomyelitis (EAE) | Within brain lesions | 0.4–3% | Mice | [ |
| Systemic lupus (SLE, juvenile) | CD15+ low density granulocytes in circulation | 10% | Human | [ |
Example concentrations of cytokines and chemokines in the microenvironment.
| Cancer (breast, pg/mL/mg)a | RA (SFb, pg/mL) | MS/EAE (CSFc, pg/mL) | SLE (serum, pg/mL) | ||
|---|---|---|---|---|---|
| IL-1 | Disease | 2.7–3.5 [ | 2.6 [ | 0.02 [ | 0.24 [ |
| Healthy/remission | 0 [ | 0 [ | 0 [ | 0.1 [ | |
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| TNF | Disease | 7.2 [ | 14.0 [ | 1.85 [ | 0.34 [ |
| Healthy/remission | 1.6 [ | 3.5 [ | 0.93 [ | 0.1–2.2 [ | |
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| IFN | Disease | 27.6 [ | 0 [ | 3.27 [ | 0.64 [ |
| Healthy/remission | 16.6 [ | 0–3.5 [ | 0.2–0.52 [ | 1.3–11.7 [ | |
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| IL-17A | Disease | 0 [ | 0 [ | 6.93 [ | 97.42 [ |
| Healthy/remission | 0 [ | 0 [ | 3.36 [ | 3.30 [ | |
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| IL-6 | Disease | 17.2 [ | 1,253 [ | 2.86 [ | 10.02 [ |
| Healthy/remission | 1.2 [ | 1,170 [ | 2.5–12 [ | 0.5–2.18 [ | |
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| TGF | Disease | 86.7 [ | 768 [ | 74.6 [ | 42,990 [ |
| Healthy/remission | 0 [ | 64 [ | 82,710 [ | ||
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| IL-10 | Disease | 0.3 [ | 16.2 [ | 0.95 [ | 1.2 [ |
| Healthy/remission | 0 [ | 0 [ | 0–0.63 | 0.54 [ | |
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| CCL2/MCP-1 | Disease | 121 [ | 25,000 [ | 116.3 [ | 136 [ |
| Healthy/remission | 1.9 [ | 920–2900 [ | 163–526 [ | 71 [ | |
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| VEGF | Disease | 1,148 [ | 1,100 [ | Below the level of detection [ | 300.8 [ |
| Healthy/remission | 163 [ | 700 [ | Below the level of detection [ | 124 [ | |
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| IL-4 | Disease | 1.7–3.1 [ | 0 [ | 0.17 [ | 0.1–0.2 [ |
| Healthy/remission | 0 [ | 0 [ | 0.03–0.1 [ |
0 | |
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| IL-8 | Disease | 68 [ | 584 [ | 30–35 [ | 358 [ |
| Healthy/remission | 1 [ | 451 [ | 28–31 [ | 150 [ | |
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| IL-12 | Disease | 2.3 [ | 10.5 [ | 1.44 [ | 1.0 [ |
| Healthy/remission | 1.4 [ | 6.1 [ | 0.56–1.4 [ | 0.18 [ | |
aMeasured in tumor extracts.
bMeasured in the synovial fluid (SF).
cMeasured in the cerebrospinal fluid (CSF).